Search CORE

3 research outputs found

Supplemental Information 10: Antigenic determinants of Gal/GalNAc lectin

Author: Arias
Bansal
Centres for Disease Control and Prevention
Cheng
Clark
Colovos
García
Ghosh
Hooft
Kelley
Khairnar
Koushik
Laskowski
Luthy
Mukherjee
Parija
Pontius
Quach
Rasti
Ravdin
Roy
Stanley
Stanley Jr
Stephen
Sultan
Teixeira
Yang
Zhang
Publication venue: 'PeerJ'
Publication date
Field of study

A Network-Based Multi-Target Computational Estimation Scheme for Anticoagulant Activities of Compounds

Author: A Bender
A Bender
A Kontijevskis
A Kranjc
A Mitsos
A Stephanou
AD Wist
AG Olivero
BK Shoichet
BL Davidson
C Auffray
Canghai Li
CB Wu
CS Shi
D Ricklin
DS Wishart
E Jenwitheesuk
E Papagrigoriou
EW Davie
F Dullweber
F Tan
G Joshi-Tope
GV Paolini
H Geppert
H Kitano
H Kitano
H Nishio
H Park
H Sun
J Emsley
J Mestres
J Tang
JCK Ngo
JL Jenkins
Jun Song
Jörg Langowski
K Krupinski
KG Mann
KG Zbinden
KI Goh
KP Hopfner
KR Guertin
L Wei
Lirong Chen
M Adler
M Di Nisio
MA Yildirim
MD Huang
MJ Keiser
MK Sakharkar
O Ortolani
P Csermely
P Stephen
Qian Li
R Jiang
R Rai
S Schuster
SJ Everse
TA Halgren
TJ Tucker
TS Korcsmáros
U Rester
V Agoston
V Latora
VC Yee
XB Qiao
XD Li
Xiaojie Xu
Xudong Li
Y Li
Y Satoh
Yalin Tang
Z Spiro
Publication venue: Public Library of Science
Publication date: 01/01/2011
Field of study

BACKGROUND: Traditional virtual screening method pays more attention on predicted binding affinity between drug molecule and target related to a certain disease instead of phenotypic data of drug molecule against disease system, as is often less effective on discovery of the drug which is used to treat many types of complex diseases. Virtual screening against a complex disease by general network estimation has become feasible with the development of network biology and system biology. More effective methods of computational estimation for the whole efficacy of a compound in a complex disease system are needed, given the distinct weightiness of the different target in a biological process and the standpoint that partial inhibition of several targets can be more efficient than the complete inhibition of a single target. METHODOLOGY: We developed a novel approach by integrating the affinity predictions from multi-target docking studies with biological network efficiency analysis to estimate the anticoagulant activities of compounds. From results of network efficiency calculation for human clotting cascade, factor Xa and thrombin were identified as the two most fragile enzymes, while the catalytic reaction mediated by complex IXa:VIIIa and the formation of the complex VIIIa:IXa were recognized as the two most fragile biological matter in the human clotting cascade system. Furthermore, the method which combined network efficiency with molecular docking scores was applied to estimate the anticoagulant activities of a serial of argatroban intermediates and eight natural products respectively. The better correlation (r = 0.671) between the experimental data and the decrease of the network deficiency suggests that the approach could be a promising computational systems biology tool to aid identification of anticoagulant activities of compounds in drug discovery. CONCLUSIONS: This article proposes a network-based multi-target computational estimation method for anticoagulant activities of compounds by combining network efficiency analysis with scoring function from molecular docking

Directory of Open Access Journals

Evaluation of Trypanosoma brucei asparagine synthetase A and ribose 5-phosphate isomerase B as potential drug targets

Author: Inês Marina Soares Loureiro
Publication venue
Publication date: 05/05/2015
Field of study